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Construction of the Gypsum-Coated Scaffolds for In Situ Bone Regeneration

机译:用于原位骨再生的石膏涂层支架的构建

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It is significant to use functional biomaterials to rationally engineer microenvironments for in situ bone regeneration in the field of bone tissue engineering. To this end, we constructed the gypsum-coated β-tricalcium phosphate (G-TCP) scaffolds by combing a three-dimensional printing technique and an epitaxial gypsum growth method. In vitro simulation experiments showed that the as-prepared scaffolds could establish a dynamic and weakly acidic microenvironment in a simulated body liquid, in which the pH and the calcium ion concentration always changed due to the gypsum degradation and growth of bone-like apatite nanoplates on the scaffold surfaces. The cell experiments confirmed that the microenvironment established by the G-TCP surfaces promoted rapid osteogenic differentiation and proliferation of bone marrow mesenchymal stem cells (BM-MSCs). In vivo experiments confirmed that the G-TCP scaffolds had high bioactivity in modulating in situ regeneration of bone, and the bioactivity of the G-TCP scaffolds was endowed by correct pore structures, degradation of gypsum, and growth of a bone-like apatite layer. The microenvironment established by the gypsum degradation could stimulate tissue inflammation and recruit white blood cells and BM-MSCs and thus accelerating native healing cascades of the bone defects via a bone growth/remodeling–absorption cycle process. Furthermore, in vivo experiments demonstrated that after the bone defects had healed completely, the as-prepared scaffolds also degraded completely within 24 weeks.
机译:在骨组织工程领域,利用功能性生物材料合理构建原位骨再生微环境具有重要意义。为此,我们结合三维打印技术和外延石膏生长方法构建了石膏涂层β-磷酸三钙(G-TCP)支架。体外模拟实验表明,所制备的支架可以在模拟体液中建立一个动态的弱酸性微环境,由于石膏的降解和支架表面类骨磷灰石纳米板的生长,pH值和钙离子浓度总是发生变化。细胞实验证实,G-TCP表面建立的微环境促进了骨髓间充质干细胞(BM-MSCs)的快速成骨分化和增殖。体内实验证实,G-TCP支架在调节骨原位再生方面具有很高的生物活性,并且G-TCP支架的生物活性是由正确的孔结构、石膏降解和类骨磷灰石层的生长赋予的。石膏降解形成的微环境可以刺激组织炎症,招募白细胞和BM-MSC,从而通过骨生长/重塑-吸收循环过程加速骨缺损的自然愈合级联。此外,体内实验表明,在骨缺损完全愈合后,制备的支架也在24周内完全降解。

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